Cold Spring Harbor molecular case studies, volume 9, issue 4, pages a006318

PD-L1+diffuse large B-cell lymphoma with extremely high mutational burden and microsatellite instability due to acquiredPMS2mutation

Publication typeJournal Article
Publication date2023-12-01
scimago Q2
SJR0.801
CiteScore3.2
Impact factor1.8
ISSN23732873, 23732865
PubMed ID:  38199780
General Medicine
Abstract

We present a unique case of a single patient presenting with two mutationally distinct, PD-L1+diffuse large B-cell lymphomas (DLBCLs). One of these DLBCLs demonstrated exceptionally high mutational burden (eight disease-associated variants and 41 variants of undetermined significance) with microsatellite instability (MSI) and an acquiredPMS2mutation with loss of PMS2 protein expression, detected postchemotherapy. This report, while highlighting the extent of possible tumor heterogeneity across separate clonal expansions as well as possible syndromic B-cell neoplasia, supports the notion that, although rare, PD-L1 expression and associated states permissive of high mutational burden (such as mismatch repair gene loss of function/MSI) should be more routinely considered in DLBCLs. Appropriate testing may be predictive of outcome and inform the utility of targeted therapy in these genetically diverse and historically treatment-refractory malignancies.

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